Evaluation of acetamiprid and azoxystrobin residues and their hormonal disrupting effects on male rats using liquid chromatography-tandem mass spectrometry

Acetamiprid (neonicotinoid insecticide) and azoxystrobin (fungicide) are widespread pesticides used for pest management, but they have the potential for toxicity to mammals. The goal of this study was to look for oxidative stress, metabolic alterations, and reproductive problems in male rats’ serum after 2 months of exposure to sub-lethal dosages of acetamiprid and azoxystrobin. Seven classes of male rats were formed: control, 3 groups of acetamiprid (1/10, 1/20, 1/40 LD50), and 3 groups of azoxystrobin (1/10, 1/20, 1/40 LD50) and were orally daily treated (n = 8/group). Our findings revealed that acetamiprid and azoxystrobin disrupted oxidative and metabolic processes in the examined rats throughout 30 and 60 days of testing. The levels of nitric oxide increased significantly, while catalase, a superoxide dismutase enzyme, and glutathione reductase activity were reduced. Serum levels of sex hormones, calcium, and total protein have all dropped substantially in rats. In comparison to the control group, the testis and liver structure, as well as spermatozoa parameters, had distinct histological characteristics. In conclusion, acetamiprid and azoxystrobin exhibit dose- and time-dependent effects on oxidative parameters that cause testis damage.

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Mechanisms and histopathological impacts of acetamiprid and azoxystrobin in male rats

El-Hak

Al-Eisa

Ryad

et al. 2022

Environ Sci Pollut Res

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Salimi

Asadikaram

Abolhassani

et al. 2023

Environ Sci Pollut Res

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Evaluation of acetamiprid and azoxystrobin residues and their hormonal disrupting effects on male rats using liquid chromatography-tandem mass spectrometry

Cited by 4 publications

References 43 publications

Mechanisms and histopathological impacts of acetamiprid and azoxystrobin in male rats

Mechanisms and histopathological impacts of acetamiprid and azoxystrobin in male rats

Organochlorine pesticides induce thyroid tumors through oxidative stress; an in vivo and in silico study

Comparison of prenatal and postnatal exposure to neonicotinoids and their temporal trends in breast milk

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